Your search keyword '"Fogal SE"' showing total 8 results

1. NFAM1 Promotes Pro-Inflammatory Cytokine Production in Mouse and Human Monocytes.

Author

Juchem KW, Gounder AP, Gao JP, Seccareccia E, Yeddula N, Huffmaster NJ, Côté-Martin A, Fogal SE, Souza D, Wang SS, Glynn ERA, Yung I, Ritchie J, Li L, Zheng J, Mbow ML, Li J, and Chanda SK

Subjects

Animals, B-Lymphocytes immunology, CD40 Antigens immunology, CD40 Ligand immunology, Cells, Cultured, Colitis, Ulcerative immunology, Crohn Disease immunology, Humans, Inflammatory Bowel Diseases immunology, Interleukin-12 immunology, Intestinal Mucosa immunology, Male, Mice, Mice, Transgenic, Neutrophils immunology, Signal Transduction immunology, T-Lymphocytes immunology, Tumor Necrosis Factor-alpha immunology, Cytokines immunology, Inflammation immunology, Membrane Proteins immunology, Monocytes immunology

Abstract

NFAT activating protein with ITAM motif 1 (NFAM1) is an ITAM bearing-transmembrane receptor that has been reported to play a role in B cell signaling and development. We performed expression analysis of NFAM1 using publicly available gene expression data sets and found that NFAM1 expression is significantly induced in intestinal biopsies from Crohn's disease (CD) and ulcerative colitis (UC) patients. At the cellular level, we further observed high expression of NFAM1 in monocytes and neutrophils, and low expression in B and T cells. To explore the role of NFAM1 in multiple immune cells and its potential role in IBD, we generated NFAM1 -/- mice. In contrast with previous reports using NFAM1-transgenic mice, NFAM1 -/- mice have no obvious defects in immune cell development, or B cell responses. Interestingly, NFAM1 -/- monocytes produce reduced levels of TNF-α in response to activation by multiple IBD-relevant stimuli, including CD40L, TLR ligands and MDP. Additional cytokines and chemokines such as IL-6, IL-12, CCL3 and CCL4 are also reduced in CD40L stimulated NFAM1 -/- monocytes. Collectively, these findings indicate that NFAM1 promotes monocyte activation, thereby amplifying the response to diverse stimuli. Similarly, we observed that deletion of NFAM1 in human monocytes reduces expression of CD40L-induced CCL4. Lastly, to assess the role of NFAM1 in IBD, we compared development of anti-CD40 induced colitis in NFAM1 +/+ and NFAM1 -/- mice. We found that although NFAM1 deletion had no impact on development of gut pathology, we did observe a decrease in serum TNF-α, confirming that NFAM1 promotes pro-inflammatory cytokine production in vivo . Taken together, we conclude that NFAM1 functions to amplify cytokine production and should be further evaluated as a therapeutic target for treatment of autoimmune disease., Competing Interests: SC served as Principal Investigator of the contract. KWJ, JPG, ES, ACM, SEF, DS, SSW, ERAG, IY, JR, LL, JZ, MLM and JL were employees of Boehringer Ingelheim. The authors disclose that financial support for this project was provided by Boehringer Ingelheim via a research contract to Sanford Burnham Prebys Medical Discovery Institute. Boehringer Ingelheim had the following involvement with the study: experimental design, data acquisition, analysis and writing the paper., (Copyright © 2022 Juchem, Gounder, Gao, Seccareccia, Yeddula, Huffmaster, Côté-Martin, Fogal, Souza, Wang, Glynn, Yung, Ritchie, Li, Zheng, Mbow, Li and Chanda.)

Published

2022

2. The potent and selective RIPK2 inhibitor BI 706039 improves intestinal inflammation in the TRUC mouse model of inflammatory bowel disease.

Author

Ermann J, Matmusaev M, Haley EK, Braun C, Jost F, Mayer-Wrangowski S, Hsiao P, Ting N, Li L, Terenzio D, Chime J, Lukas S, Patnaude L, Panzenbeck M, Csordas D, Zheng J, Mierz D, Simpson T, King FJ, Klimowicz AP, Mbow ML, Fine JS, Miller CA, Fogal SE, and Byrne FR

Subjects

Animals, Biological Availability, Cells, Cultured, Colitis, Ulcerative enzymology, Colitis, Ulcerative genetics, Colitis, Ulcerative pathology, Colon enzymology, Colon pathology, Crohn Disease enzymology, Crohn Disease pathology, Cytokines genetics, Cytokines metabolism, DNA-Binding Proteins genetics, Disease Models, Animal, Feces chemistry, Humans, Inflammation Mediators metabolism, Lipocalins metabolism, Mice, Inbred BALB C, Mice, Knockout, Models, Biological, Monocytes drug effects, Monocytes metabolism, Protein Kinase Inhibitors pharmacokinetics, Receptor-Interacting Protein Serine-Threonine Kinase 2 genetics, Receptor-Interacting Protein Serine-Threonine Kinase 2 metabolism, T-Box Domain Proteins genetics, Mice, T-bet Transcription Factor, Colitis, Ulcerative drug therapy, Colon drug effects, Protein Kinase Inhibitors pharmacology, Receptor-Interacting Protein Serine-Threonine Kinase 2 antagonists & inhibitors

Abstract

Mouse and human data implicate the NOD1 and NOD2 sensors of the intestinal microbiome and the associated signal transduction via the receptor interacting protein kinase 2 (RIPK2) as a potential key signaling node for the development of inflammatory bowel disease (IBD) and an attractive target for pharmacological intervention. The TRUC mouse model of IBD was strongly indicated for evaluating RIPK2 antagonism for its effect on intestinal inflammation based on previous knockout studies with NOD1, NOD2, and RIPK2. We identified and profiled the BI 706039 molecule as a potent and specific functional inhibitor of both human and mouse RIPK2 and with favorable pharmacokinetic properties. We dosed BI 706039 in the spontaneous TRUC mouse model from age 28 to 56 days. Oral, daily administration of BI 706039 caused dose-responsive and significant improvement in colonic histopathological inflammation, colon weight, and terminal levels of protein-normalized fecal lipocalin (all P values <0.001). These observations correlated with dose responsively increasing systemic levels of the BI 706039 compound, splenic molecular target engagement of RIPK2, and modulation of inflammatory genes in the colon. This demonstrates that a relatively low oral dose of a potent and selective RIPK2 inhibitor can modulate signaling in the intestinal immune system and significantly improve disease associated intestinal inflammation. NEW & NOTEWORTHY The RIPK2 kinase at the apex of microbiome immunosensing is an attractive target for pharmacological intervention. A low oral dose of a RIPK2 inhibitor leads to significantly improved intestinal inflammation in the murine TRUC model of colitis. A selective and potent inhibitor of the RIPK2 kinase may represent a new class of therapeutics that target microbiome-driven signaling for the treatment of IBD.

Published

2021

3. CCR1 plays a critical role in modulating pain through hematopoietic and non-hematopoietic cells.

Author

Lewis ND, Muthukumarana A, Fogal SE, Corradini L, Stefanopoulos DE, Adusumalli P, Pelletier J, Panzenbeck M, Berg K, Canfield M, Cook BN, Razavi H, Kuzmich D, Anderson S, Allard D, Harrison P, Grimaldi C, Souza D, Harcken C, Fryer RM, Modis LK, and Brown ML

Subjects

Acetic Acid, Animals, Arthritis, Experimental genetics, Arthritis, Experimental immunology, Bone Marrow Cells immunology, Bone Marrow Cells metabolism, Bone Marrow Transplantation methods, Cell Movement genetics, Cell Movement immunology, Flow Cytometry, Freund's Adjuvant, Hyperalgesia chemically induced, Hyperalgesia genetics, Hyperalgesia immunology, Leukocytes immunology, Leukocytes metabolism, Mice, Inbred C57BL, Mice, Knockout, Myeloid Cells immunology, Myeloid Cells metabolism, Neutrophil Infiltration genetics, Neutrophils metabolism, Pain chemically induced, Pain genetics, Pain Measurement methods, Peritonitis genetics, Peritonitis immunology, Peritonitis metabolism, Receptors, CCR1 antagonists & inhibitors, Receptors, CCR1 genetics, Neutrophil Infiltration immunology, Neutrophils immunology, Pain immunology, Receptors, CCR1 immunology

Abstract

Inflammation is associated with immune cells infiltrating into the inflammatory site and pain. CC chemokine receptor 1 (CCR1) mediates trafficking of leukocytes to sites of inflammation. However, the contribution of CCR1 to pain is incompletely understood. Here we report an unexpected discovery that CCR1-mediated trafficking of neutrophils and CCR1 activity on non-hematopoietic cells both modulate pain. Using a genetic approach (CCR1-/- animals) and pharmacological inhibition of CCR1 with selective inhibitors, we show significant reductions in pain responses using the acetic acid-induced writhing and complete Freund's adjuvant-induced mechanical hyperalgesia models. Reductions in writhing correlated with reduced trafficking of myeloid cells into the peritoneal cavity. We show that CCR1 is highly expressed on circulating neutrophils and their depletion decreases acetic acid-induced writhing. However, administration of neutrophils into the peritoneal cavity did not enhance acetic acid-induced writhing in wild-type (WT) or CCR1-/- mice. Additionally, selective knockout of CCR1 in either the hematopoietic or non-hematopoietic compartments also reduced writhing. Together these data suggest that CCR1 functions to significantly modulate pain by controlling neutrophil trafficking to the inflammatory site and having an unexpected role on non-hematopoietic cells. As inflammatory diseases are often accompanied with infiltrating immune cells at the inflammatory site and pain, CCR1 antagonism may provide a dual benefit by restricting leukocyte trafficking and reducing pain.

Published

2014

4. Immunodominant T-cell epitopes of MOG reside in its transmembrane and cytoplasmic domains in EAE.

Author

Shetty A, Gupta SG, Varrin-Doyer M, Weber MS, Prod'homme T, Molnarfi N, Ji N, Nelson PA, Patarroyo JC, Schulze-Topphoff U, Fogal SE, Forsthuber T, Sobel RA, Bernard CC, Slavin AJ, and Zamvil SS

Abstract

Objective: Studies evaluating T-cell recognition of myelin oligodendrocyte glycoprotein (MOG) in multiple sclerosis (MS) and its model, experimental autoimmune encephalomyelitis (EAE), have focused mostly on its 117 amino acid (aa) extracellular domain, especially peptide (p) 35-55. We characterized T-cell responses to the entire 218 aa MOG sequence, including its transmembrane and cytoplasmic domains., Methods: T-cell recognition in mice was examined using overlapping peptides and intact full-length mouse MOG. EAE was evaluated by peptide immunization and by adoptive transfer of MOG epitope-specific T cells. Frequency of epitope-specific T cells was examined by ELISPOT., Results: Three T-cell determinants of MOG were discovered in its transmembrane and cytoplasmic domains, p119-132, p181-195, and p186-200. Transmembrane MOG p119-132 induced clinical EAE, CNS inflammation, and demyelination as potently as p35-55 in C57BL/6 mice and other H-2(b) strains. p119-128 contained its minimal encephalitogenic epitope. p119-132 did not cause disease in EAE-susceptible non-H-2(b) strains, including Biozzi, NOD, and PL/J. MOG p119-132-specific T cells produced Th1 and Th17 cytokines and transferred EAE to wild-type recipient mice. After immunization with full-length MOG, a significantly higher frequency of MOG-reactive T cells responded to p119-132 than to p35-55, demonstrating that p119-132 is an immunodominant encephalitogenic epitope. MOG p181-195 did not cause EAE, and MOG p181-195-specific T cells could not transfer EAE into wild-type or highly susceptible T- and B-cell-deficient mice., Conclusions: Transmembrane and cytoplasmic domains of MOG contain immunodominant T-cell epitopes in EAE. A CNS autoantigen can also contain nonpathogenic stimulatory T-cell epitopes. Recognition that a myelin antigen contains multiple encephalitogenic and nonencephalitogenic determinants may have implications for therapeutic development in MS.

Published

2014

5. Circulating monocytes are reduced by sphingosine-1-phosphate receptor modulators independently of S1P3.

Author

Lewis ND, Haxhinasto SA, Anderson SM, Stefanopoulos DE, Fogal SE, Adusumalli P, Desai SN, Patnaude LA, Lukas SM, Ryan KR, Slavin AJ, Brown ML, and Modis LK

Subjects

Animals, Bone Marrow drug effects, Bone Marrow metabolism, Cell Movement immunology, Cytokines biosynthesis, Encephalomyelitis, Autoimmune, Experimental immunology, Encephalomyelitis, Autoimmune, Experimental metabolism, Female, Fingolimod Hydrochloride, Killer Cells, Natural metabolism, Leukocyte Count, Mice, Monocytes immunology, Neutrophils metabolism, Rats, Sphingosine pharmacology, Spleen drug effects, Spleen metabolism, Monocytes drug effects, Monocytes metabolism, Propylene Glycols pharmacology, Receptors, Lysosphingolipid metabolism, Sphingosine analogs & derivatives

Abstract

Sphingosine-1-phosphate (S1P) receptors are critical for lymphocyte egress from secondary lymphoid organs, and S1P receptor modulators suppress lymphocyte circulation. However, the role of S1P receptors on monocytes is less clear. To elucidate this, we systematically evaluated monocytes in rats and mice, both in naive and inflammatory conditions, with S1P receptor modulators FTY720 and BAF312. We demonstrate that S1P receptor modulators reduce circulating monocytes in a similar time course as lymphocytes. Furthermore, total monocyte numbers were increased in the spleen and bone marrow, suggesting that S1P receptor modulation restricts egress from hematopoietic organs. Monocytes treated ex vivo with FTY720 had reduced CD40 expression and TNF-α production, suggesting a direct effect on monocyte activation. Similar reductions in protein expression and cytokine production were also found in vivo. Suppression of experimental autoimmune encephalomyelitis in mice and rats by FTY720 correlated with reduced numbers of lymphocytes and monocytes. These effects on monocytes were independent of S1P3, as treatment with BAF312, a S1P1,4,5 modulator, led to similar results. These data reveal a novel role for S1P receptors on monocytes and offer additional insights on the mechanism of action of S1P receptor modulators in disease.

Published

2013

6. Small molecule LFA-1 antagonists compete with an anti-LFA-1 monoclonal antibody for binding to the CD11a I domain: development of a flow-cytometry-based receptor occupancy assay.

Author

Woska JR Jr, Last-Barney K, Rothlein R, Kroe RR, Reilly PL, Jeanfavre DD, Mainolfi EA, Kelly TA, Caviness GO, Fogal SE, Panzenbeck MJ, Kishimoto TK, and Giblin PA

Subjects

Animals, Antibodies, Monoclonal immunology, Antibody Specificity immunology, Binding, Competitive, CD11a Antigen immunology, Cell Adhesion Molecules immunology, Cell Adhesion Molecules physiology, Humans, Imidazoles pharmacology, Lymphocyte Function-Associated Antigen-1 metabolism, Lymphocytes immunology, Lymphocytes metabolism, Neutrophils immunology, Neutrophils metabolism, Pan troglodytes, Receptors, Leukocyte-Adhesion immunology, Receptors, Leukocyte-Adhesion physiology, Saimiri, Antibodies, Monoclonal metabolism, CD11a Antigen metabolism, Flow Cytometry methods, Imidazoles metabolism, Imidazolidines, Lymphocyte Function-Associated Antigen-1 immunology

Abstract

The beta(2) integrin LFA-1 (CD11a/CD18) is a leukocyte-specific adhesion molecule that mediates leukocyte extravasation, antigen presentation, and T-cell-mediated cytolysis through its interaction with its counter-receptors, ICAM-1, ICAM-2, and ICAM-3. We have recently described a small molecule antagonist of LFA-1 (BIRT 377) that inhibits LFA-1/ICAM-1 molecular interactions, LFA-1-dependent adhesion assays, antigen-induced proliferation of T-cells, and superantigen-induced production of IL-2 in vivo in mice. We have also recently described a unique monoclonal antibody, R3.1, which competes with BIRT 377 and its analogs for binding to both purified full-length LFA-1 and the purified recombinant I domain module. In this manuscript, we extend these studies to cell-based systems and utilize this unique reagent for the development of a receptor occupancy assay. Exploiting these observations, we have designed and validated an assay that allows us to measure receptor occupancy in vitro on monkey and human peripheral blood leukocytes and ex vivo in whole blood from monkeys dosed with small molecule LFA-1 antagonists. Further refinement of these reagents has led to the development of a Fab-based assay that allows rapid and reproducible analysis of whole blood samples. These optimized reagents allow for quantification of the number of receptors expressed on the cell surface and a more accurate quantitation of receptor occupancy.

Published

2003

7. Lipid-based delivery systems for improving the bioavailability and lymphatic transport of a poorly water-soluble LTB4 inhibitor.

Author

Hauss DJ, Fogal SE, Ficorilli JV, Price CA, Roy T, Jayaraj AA, and Keirns JJ

Subjects

Administration, Oral, Analysis of Variance, Animals, Area Under Curve, Benzoxazoles blood, Benzoxazoles chemistry, Biological Availability, Chylomicrons chemistry, Drug Carriers, Emulsions pharmacokinetics, Excipients chemistry, Glycerides chemistry, Half-Life, Injections, Intravenous, Intestinal Absorption physiology, Male, Rats, Rats, Inbred Strains, Solubility, Soybean Oil chemistry, Suspensions pharmacokinetics, Benzoxazoles pharmacokinetics, Leukotriene B4 antagonists & inhibitors, Lymphatic System metabolism, Triglycerides metabolism

Abstract

Ontazolast is a potent inhibitor (IC50 = 1 nm) of calcium ionophore A23187-stimulated leukotriene B4 (LTB4) biosynthesis in human peripheral blood leukocytes. The compound is practically insoluble in water (0.14 microgram/mL) and previous studies in animals have demonstrated extensive presystemic drug clearance through hepatic first-pass metabolism. Bioavailability of a suspension formulation in rats was less than 1%, but increased to approximately 9% when administered as a 20% soybean oil-in-water emulsion. The emulsion formulation and three additional lipid-based formulations were administered by gavage to conscious, minimally restrained rats in a novel, double-cannulated model to determine the effects of formulation on systemic blood absorption and mesenteric lymph transport of ontazolast. The bioavailability of ontazolast was significantly and substantially enhanced by all of the lipid-based formulations. While these formulations also significantly increased the amount of ontazolast transported by the lymph, the total amounts transported were insufficient to account for the improvement in bioavailability, which may be due to the elimination or reduction of the barriers of poor aqueous solubility and slow dissolution to absorption of ontazolast from the gastrointestinal tract, or the effects of lipid on the gastrointestinal membrane permeability, transit time, or metabolism of ontazolast. Semisolid SEDDS formulations, composed of Peceol and Gelucire 44/14, produced bioavailability similar to the emulsion formulation. The total amount of ontazolast transported by the lymph varied directly with the amount of concurrent triglyceride transport and appeared to be favored by formulations that prolong gastric emptying time or promote rapid absorption of ontazolast from the gastrointestinal tract.

Published

1998

8. Captopril-induced hypotension is inhibited by the bradykinin blocker HOE-140 in Na(+)-depleted marmosets.

Author

Panzenbeck MJ, Loughnan CL, Madwed JB, Winquist RJ, and Fogal SE

Subjects

Administration, Oral, Animals, Blood Pressure drug effects, Bradykinin pharmacology, Callithrix, Captopril pharmacology, Female, Hypotension physiopathology, Injections, Subcutaneous, Male, Piperazines pharmacology, Renin antagonists & inhibitors, Sodium metabolism, Thiazoles pharmacology, Bradykinin analogs & derivatives, Bradykinin antagonists & inhibitors, Captopril antagonists & inhibitors, Hypotension chemically induced, Sodium deficiency

Abstract

Inhibition of angiotensin-converting enzyme (ACE) inhibits formation of angiotensin II and, by inhibition of kinin metabolism, may also increase vascular bradykinin. The present experiments were done in sodium-depleted, conscious, unrestrained marmosets (n = 5-11) to examine the contribution of bradykinin to ACE inhibitor-induced hypotension. Aortic blood pressure and heart rate (HR) were monitored via telemetry. After sodium depletion (low-sodium diet and furosemide), captopril (1 mg/kg po) caused a significant (P < 0.05) decrease in mean arterial blood pressure (MABP) (-34 +/- 3 mmHg, maximally, from 79 +/- 2 mmHg) but no change in HR compared with vehicle treatment. The bradykinin receptor antagonist HOE-140 (1 mg/kg sc) significantly inhibited the hypotensive response to captopril and caused marked tachycardia (+133 +/- 14 beats/min from 214 +/- 8 beats/min). HOE-140 (1 mg/kg sc) followed by vehicle administration had no effect on MABP but increased HR similarly. The hypotensive response to captopril was inhibited by HOE-140 regardless of the order of administration or the route of captopril administration (by mouth vs. subcutaneously). The hypotensive response to a renin inhibitor, A-72517 (3 mg/kg sc), was not inhibited by prior HOE-140 administration despite a similar HOE-140-induced tachycardia. These data suggest that the hypotensive effect of captopril in sodium-depleted, conscious marmosets is dependent on functional bradykinin B2 receptors. Also, blockade of B2 receptors uncovers marked tachycardia in this model, suggesting a tonic effect of bradykinin on control of HR in marmosets.

Published

1995